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肝细胞核因子3参与胚胎干细胞的内胚层分化

Involvement of hepatocyte nuclear factor 3 in endoderm differentiation of embryonic stem cells.

作者信息

Levinson-Dushnik M, Benvenisty N

机构信息

Department of Genetics, Institute of Life Sciences, The Hebrew University of Jerusalem, Givat-Ram, Israel.

出版信息

Mol Cell Biol. 1997 Jul;17(7):3817-22. doi: 10.1128/MCB.17.7.3817.

Abstract

The transcription factors of the hepatocyte nuclear factor 3 (HNF3) family, which are active in the liver, are expressed early during endoderm differentiation. To study their involvement in early murine development, we examined their role in embryonic stem (ES) cells. HNF3alpha or HNF3beta mRNA transcripts were not detected in ES cells before differentiation, and only low levels of HNF3beta mRNA were detected at a late stage of differentiation of ES cells to embryoid bodies (EB) (20 days after induction of differentiation). To examine the consequences of overexpressing HNF3alpha or -beta in ES cells, we transfected the two genes into these cells and determined the levels of expression of tissue-specific genes during EB differentiation. Specifically, we examined expression of albumin, cystic fibrosis transmembrane conductance regulator (CFTR), phosphoenolpyruvate carboxykinase (PEPCK), alpha1-antitrypsin, transthyretin, zeta-globin, and neurofilament 68kd as markers for different cell lineages. Overexpression of HNF3beta (and to a lesser extent of HNF3alpha) induced the expression of genes associated with endodermal lineage, namely, the genes for CFTR and albumin, but did not induce the expression of genes involved in late endoderm differentiation, such as the genes for PEPCK and alpha1-antitrypsin. Moreover, expression of HNF1beta was highly induced in HNF3-overexpressing cells, while expression of HNF1alpha and HNF4 was only mildly induced in these cells. Therefore, HNF3alpha and -beta seem to be involved in early endoderm differentiation of ES cells and together with other developmental factors are apparently needed for the induction of the endodermal lineage in vivo.

摘要

在肝脏中具有活性的肝细胞核因子3(HNF3)家族转录因子,在内胚层分化早期就开始表达。为了研究它们在小鼠早期发育中的作用,我们检测了它们在胚胎干细胞(ES细胞)中的作用。在分化前的ES细胞中未检测到HNF3α或HNF3β mRNA转录本,在ES细胞分化为胚状体(EB)的后期(诱导分化20天后)仅检测到低水平的HNF3β mRNA。为了检测在ES细胞中过表达HNF3α或-β的后果,我们将这两个基因转染到这些细胞中,并测定了EB分化过程中组织特异性基因的表达水平。具体来说,我们检测了白蛋白、囊性纤维化跨膜传导调节因子(CFTR)、磷酸烯醇丙酮酸羧激酶(PEPCK)、α1-抗胰蛋白酶、转甲状腺素蛋白、ζ-珠蛋白和神经丝68kd的表达,作为不同细胞谱系的标志物。HNF3β的过表达(以及程度较轻的HNF3α的过表达)诱导了与内胚层谱系相关的基因的表达,即CFTR和白蛋白的基因,但没有诱导参与内胚层晚期分化的基因的表达,如PEPCK和α1-抗胰蛋白酶的基因。此外,HNF1β的表达在HNF3过表达的细胞中被高度诱导,而HNF1α和HNF-4的表达在这些细胞中仅被轻度诱导。因此,HNF3α和-β似乎参与了ES细胞的早期内胚层分化,并且与其他发育因子一起显然是体内诱导内胚层谱系所必需的。

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